Determination of plasma soluble fibrin using a new ELISA method in patients with disseminated intravascular coagulation

We measured plasma levels of soluble fibrin (SF) In 98 patients suspected of having disseminated intravascuiar coagulation (DIC) using a newly developed enzyme-linked immunosorbent assay (ELISA) and investigated the correlations between SF determinations and measurements of other hemostatic molecular markers to determine the diagnostic usefulness of determinations of SF. Patients were classified into four groups according to their clinical and laboratory findings: overt DIC (n = 33). subclinical DIC (n = 23). hypercoagulability (n = 22), and non-DIC (n = 20). SF levels were significantly higher in patients with overt DIC compared with the otber three groups and were significantly higher in the subclinical DIC and hypercoagulability groups compared with the non-DiC patients. SF levels Increased significantly with each increase in the clinical stage. Although levels of thrombin-antithrombin 111 complex (TAT), prothrombin fragment l + 2 (PF,+*), cross-linked fibrin degradation products (XDP), and piasmin-antipiasmin complex (PAP) were significantly increased In patients with overt DIC compared with non-DiC patients, the values of these hemostatic molecular markers did not consistently show an increase in association with advances in the disease stage. Plasma levels of SF in patients with overt DIC showed a positive correlation with levels of TAT, XDP, and FDP(E), but not with PF, , , and PAP. Analysis of receiver-operating characteristic curves showed that the sensitivity and specificity of SF were similar to those of XDP for diagnosis of DIC. The sensitivity and specificity of SF for diagnosis of overt DIC were both above 90% when the cut-off value was set at 65 kglml. Plasma levels of SF were also increased in patients with extravascular fibrin formation without DIC.

Our findings suggest that measurement of plasma levels of SF by this ELiSA method is useful for the diagnosis of DIC and the evaluation of the patient's clinical status. Q 1996 wiiay-L~SS, inc.